Your search keyword '"Gallimore, Awen"' showing total 14 results

1. Lower Humoral and Cellular Immunity Following Asymptomatic SARS-CoV-2 Infection Compared to Symptomatic Infection in Education (The ACE Cohort)

Author

Hopkins, Georgina, Gomez, Nancy, Tucis, Davis, Bartlett, Laura, Steers, Graham, Burns, Ellie, Brown, Michaela, Harvey-Cowlishaw, Tyler, Santos, Rute, Lauder, Sarah N, Scurr, Martin, Capitani, Lorenzo, Burnell, Stephanie, Rees, Tara, Smart, Kathryn, Somerville, Michelle, Gallimore, Awen, Perera, Marianne, Potts, Martin, and Metaxaki, Marina

Abstract

Purpose: Asymptomatic SARS-CoV-2 infections were widely reported during the COVID-19 pandemic, acting as a hidden source of infection. Many existing studies investigating asymptomatic immunity failed to recruit true asymptomatic individuals. Thus, we conducted a longitudinal cohort study to evaluate humoral- and cell-mediated responses to infection and vaccination in well-defined asymptomatic young adults (the Asymptomatic COVID-19 in Education [ACE] cohort). Methods: Asymptomatic testing services located at three UK universities identified asymptomatic young adults who were subsequently recruited with age- and sex-matched symptomatic and uninfected controls. Blood and saliva samples were collected after SARS-CoV-2 Wuhan infection, and again after vaccination. 51 participant’s anti-spike antibody titres, neutralizing antibodies, and spike-specific T-cell responses were measured, against both Wuhan and Omicron B.1.1.529.1. Results: Asymptomatic participants exhibited reduced Wuhan-specific neutralization antibodies pre- and post-vaccination, as well as fewer Omicron-specific neutralization antibodies post-vaccination, compared to symptomatic participants. Lower Wuhan and Omicron-specific IgG titres in asymptomatic individuals were also observed pre- and post-vaccination, compared to symptomatic participants. There were no differences in salivary IgA levels. Conventional flow cytometry analysis and multi-dimensional clustering analysis indicated unvaccinated asymptomatic participants had significantly fewer Wuhan-specific IL-2 secreting CD4+ CD45RA+ T cells and activated CD8+ T cells than symptomatic participants, though these differences dissipated after vaccination. Conclusions: Asymptomatic infection results in decreased antibody and T cell responses to further exposure to SARS-CoV-2 variants, compared to symptomatic infection. Post-vaccination, antibody responses are still inferior, but T cell immunity increases to match symptomatic subjects, emphasising the importance of vaccination to help protect asymptomatic individuals against future variants. [ABSTRACT FROM AUTHOR]

Published

2024

2. Treg-driven tumour control by PI3Kδ inhibition limits myeloid-derived suppressor cell expansion.

Author

Lauder, Sarah N., Smart, Kathryn, Bart, Valentina M. T., Pires, Ana, Scott, Jake, Milutinovic, Stefan, Godkin, Andrew, Vanhaesebroeck, Bart, and Gallimore, Awen

Subjects

CELL physiology, IMPACT of Event Scale, RESEARCH funding, TUMORS, T cells, ANIMALS, MICE

Abstract

Background: Recent studies have demonstrated that blocking the PI3Kδ signalling enzyme (by administering a small molecule inhibitor, PI-3065) can potently improve the anti-tumour T-cell response through direct inhibition of Tregs. This treatment also has a negative impact on MDSC numbers but the primary mechanism driving this effect has remained unclear.Methods: The 4T1 breast cancer mouse model was used in combination with PI-3065 to gain insights into the effect of PI3Kδ inhibition on MDSCs.Results: PI-3065 treatment resulted in a concomitant reduction in MDSC expansion and tumour size. However, targeting Tregs independent of PI-3065 was also associated with reduced tumour volume and MDSC numbers. Surgical removal of tumours resulted in a rapid and significant decline in MDSC numbers, whilst ex vivo studies using cells from PI-3065-treated mice demonstrated no direct effect of the inhibitor on MDSC activity.Conclusions: Our data suggest that MDSCs are not inhibited directly by PI-3065 treatment but that their reduced recruitment and immunosuppression within the tumour microenvironment is an indirect consequence of PI3Kδ-inhibition-driven tumour control. This indicates that PI3Kδ inhibition drives tumour immunity by breaking down multiple immunosuppressive pathways through both direct mechanisms (on Treg) and indirect mechanisms, secondary to tumour control (on MDSCs). [ABSTRACT FROM AUTHOR]

Published

2022

3. Magnitude of venous or capillary blood-derived SARS-CoV-2-specific T cell response determines COVID-19 immunity.

Author

Scurr, Martin J., Lippiatt, George, Capitani, Lorenzo, Bentley, Kirsten, Lauder, Sarah N., Smart, Kathryn, Somerville, Michelle S., Rees, Tara, Stanton, Richard J., Gallimore, Awen, Hindley, James P., and Godkin, Andrew

Subjects

HERD immunity, COVID-19, IMMUNITY, CAPILLARIES, SARS-CoV-2, T cells

Abstract

T cells specific for SARS-CoV-2 are thought to protect against infection and development of COVID-19, but direct evidence for this is lacking. Here, we associated whole-blood-based measurement of SARS-CoV-2-specific interferon-γ-positive T cell responses with positive COVID-19 diagnostic (PCR and/or lateral flow) test results up to 6 months post-blood sampling. Amongst 148 participants donating venous blood samples, SARS-CoV-2-specific T cell response magnitude is significantly greater in those who remain protected versus those who become infected (P < 0.0001); relatively low magnitude T cell response results in a 43.2% risk of infection, whereas high magnitude reduces this risk to 5.4%. These findings are recapitulated in a further 299 participants testing a scalable capillary blood-based assay that could facilitate the acquisition of population-scale T cell immunity data (14.9% and 4.4%, respectively). Hence, measurement of SARS-CoV-2-specific T cells can prognosticate infection risk and should be assessed when monitoring individual and population immunity status. The presence of SARS-CoV-2-specific antibodies alone is not an accurate determinant of immunity. In this work, the authors investigate if whole-blood based measurement of SARS-CoV-2 specific T cell responses could prognosticate the risk of possible SARS-CoV-2 infection, and recapitulate their findings in a capillary blood-based assay. [ABSTRACT FROM AUTHOR]

Published

2022

4. Prognostic significance of interleukin-17A-producing colorectal tumour antigen-specific T cells.

Author

Thomson, Amanda, Bento, Diana F. Costa, Scurr, Martin J., Smart, Kathryn, Somerville, Michelle S., Keita, Åsa V., Gallimore, Awen, Godkin, Andrew, and Keita, Åsa V

Subjects

INTERLEUKINS, SURVIVAL, RESEARCH, RESEARCH methodology, CANCER relapse, CASE-control method, PROGNOSIS, MEDICAL cooperation, EVALUATION research, COLORECTAL cancer, INTERFERONS, COMPARATIVE studies, RESEARCH funding, TUMOR antigens, T cells, MEDICAL specialties & specialists, LONGITUDINAL method

Abstract

Background: The T cell cytokine profile is a key prognostic indicator of post-surgical outcome for colorectal cancer (CRC). Whilst TH1 (IFN-γ+) cell-mediated responses generated in CRC are well documented and are associated with improved survival, antigen-specific TH17 (IL-17A+) responses have not been similarly measured.Methods: We sought to determine the cytokine profile of circulating tumour antigen-(5T4/CEA) specific T cells of 34 CRC patients to address whether antigen-specific IL-17A responses were detectable and whether these were distinct to IFN-γ responses.Results: As with IFN-γ-producing T cells, anti-5T4/CEA TH17 responses were detectable predominantly in early stage (TNM I/II) CRC patients. Moreover, whilst IL-17A was always produced in association with IFN-γ, this release was mainly from two distinct T cell populations rather than by 'dual producing' T cells. Patients mounting both tumour-specific TH1+/TH17+ responses exhibited prolonged relapse-free survival.Conclusions: Tumour antigen-specific TH17 responses play a beneficial role in preventing post-operative colorectal tumour recurrence. [ABSTRACT FROM AUTHOR]

Published

2021

5. Primary breast tumours but not lung metastases induce protective anti-tumour immune responses after Treg-depletion.

Author

Hughes, Ellyn, Lauder, Sarah N., Smart, Kathryn, Bloom, Anja, Scott, Jake, Jones, Emma, Somerville, Michelle, Browne, Molly, Blainey, Andrew, Godkin, Andrew, Ager, Ann, and Gallimore, Awen

Subjects

IMMUNE response, SUPPRESSOR cells, TUMORS, CANCER, METASTASIS

Abstract

Although metastatic disease is responsible for the majority of cancer deaths, tests of novel immunotherapies in mouse tumour models often focus on primary tumours without determining whether these therapies also target metastatic disease. This study examined the impact of depleting Foxp3+ regulatory T cells (Treg), on lung metastases, using a mouse model of breast cancer. After Treg-depletion, generation of an immune response to the primary tumour was a critical determinant for limiting development of metastasis. Indeed, resection of the primary tumour abrogated any effect of Treg-depletion on metastases. In addition, whilst the immune response, generated by the primary tumour, prevented metastases development, it had little impact on controlling established disease. Collectively, the data indicate that metastatic cells in the lung are not controlled by immune responses induced by the primary tumour. These findings indicate that targeting Tregs alone will not suffice for treating lung metastases. [ABSTRACT FROM AUTHOR]

Published

2020

6. Sequential targeting of PI3Kδ and LAG3 as an effective anti-cancer approach.

Author

Lauder, Sarah N., Vanhaesebroeck, Bart, and Gallimore, Awen

Abstract

Emerging studies have demonstrated the potential of PI3Kδ blockade as an immunotherapy for solid tumours. In pre-clinical models, we recently demonstrated that anti-LAG3 immune checkpoint blockade vastly potentiated PI3Kδ-based immunotherapy, enabling successful tumour control in all treated mice. [ABSTRACT FROM AUTHOR]

Published

2021

7. The nature of the human T cell response to the cancer antigen 5T4 is determined by the balance of regulatory and inflammatory T cells of the same antigen-specificity: implications for vaccine design.

Author

Besneux, Matthieu, Greenshields-Watson, Alexander, Scurr, Martin J., MacLachlan, Bruce J., Christian, Adam, Davies, Michael M., Hargest, Rachel, Phillips, Simon, Godkin, Andrew, and Gallimore, Awen

Subjects

T cells, ANTIGENS, CELLS, TH1 cells, PROTEINS, COLON cancer

Abstract

The oncofoetal antigen 5T4 is a promising T cell target in the context of colorectal cancer, as demonstrated by a recent clinical study where 5T4-specific T cell responses, induced by vaccination or cyclophosphamide, were associated with a significantly prolonged survival of patients with metastatic disease. Whilst Th1-type (IFN-γ+) responses specific to 5T4, and other oncofoetal antigens, are often readily detectable in early stage CRC patients and healthy donors, their activity is suppressed as the cancer progresses by CD4+CD25hiFoxp3+ regulatory T cells (Treg) which contribute to the immunosuppressive environment conducive to tumour growth. This study mapped the fine specificity of Th1 and Treg cell responses to the 5T4 protein. Surprisingly, both immunogenic peptides and those recognised by Tregs clustered in the same HLA-DR transcending epitope-rich hotspots within the 5T4 protein. Similarly, regions of low Th1-cell immunogenicity also did not contain peptides capable of stimulating Tregs, further supporting the notion that Treg and Th1 cells recognise the same peptides. Understanding the rules which govern the balance of Th1 and Treg cells responding to a given peptide specificity is, therefore, of fundamental importance to designing strategies for manipulating the balance in favour of Th1 cells, and thus the most effective anti-cancer T cell responses. [ABSTRACT FROM AUTHOR]

Published

2019

8. Monitoring regulatory T cells in clinical samples: consensus on an essential marker set and gating strategy for regulatory T cell analysis by flow cytometry.

Author

Santegoets, Saskia, Dijkgraaf, Eveline, Battaglia, Alessandra, Beckhove, Philipp, Britten, Cedrik, Gallimore, Awen, Godkin, Andrew, Gouttefangeas, Cecile, Gruijl, Tanja, Koenen, Hans, Scheffold, Alexander, Shevach, Ethan, Staats, Janet, Taskén, Kjetil, Whiteside, Theresa, Kroep, Judith, Welters, Marij, and Burg, Sjoerd

Subjects

T cells, FLOW cytometry, BIOMARKERS, IMMUNOSUPPRESSION, CANCER immunotherapy, HEALTH outcome assessment

Abstract

Regulatory T cell (Treg)-mediated immunosuppression is considered a major obstacle for successful cancer immunotherapy. The association between clinical outcome and Tregs is being studied extensively in clinical trials, but unfortunately, no consensus has been reached about (a) the markers and (b) the gating strategy required to define human Tregs in this context, making it difficult to draw final conclusions. Therefore, we have organized an international workshop on the detection and functional testing of Tregs with leading experts in the field, and 40 participants discussing different analyses and the importance of different markers and context in which Tregs were analyzed. This resulted in a rationally composed ranking list of 'Treg markers'. Subsequently, the proposed Treg markers were tested to get insight into the overlap/differences between the most frequently used Treg definitions and their utility for Treg detection in various human tissues. Here, we conclude that the CD3, CD4, CD25, CD127, and FoxP3 markers are the minimally required markers to define human Treg cells. Staining for Ki67 and CD45RA showed to provide additional information on the activation status of Tregs. The use of markers was validated in a series of PBMC from healthy donors and cancer patients, as well as in tumor-draining lymph nodes and freshly isolated tumors. In conclusion, we propose an essential marker set comprising antibodies to CD3, CD4, CD25, CD127, Foxp3, Ki67, and CD45RA and a corresponding robust gating strategy for the context-dependent analysis of Tregs by flow cytometry. [ABSTRACT FROM AUTHOR]

Published

2015

9. TCR affinity and negative regulation limit autoimmunity.

Author

Gronski, Matthew A, Boulter, Jonathan M, Moskophidis, Demetrius, Nguyen, Linh T, Holmberg, Kaisa, Elford, Alisha R, Deenick, Elissa K, Kim, Hee O, Penninger, Josef M, Odermatt, Bernhard, Gallimore, Awen, Gascoigne, Nicholas R J, and Ohashi, Pamela S

Subjects

AUTOIMMUNE diseases, T cells, IMMUNOPATHOLOGY, PATHOGENIC microorganisms, AUTOIMMUNITY, IMMUNE response

Abstract

Autoimmune diseases are often mediated by self-reactive T cells, which must be activated to cause immunopathology. One mechanism, known as molecular mimicry, proposes that self-reactive T cells may be activated by pathogens expressing crossreactive ligands. Here we have developed a model to investigate how the affinity of the T-cell receptor (TCR) for the activating agent influences autoimmunity. Our model shows that an approximately fivefold difference in the TCR affinity for the activating ligand results in a 50% reduction in the incidence of autoimmunity. A reduction in TCR-ligand affinity to approximately 20 times lower than normal does not induce autoimmunity despite the unexpected induction of cytotoxic T lymphocytes (CTLs) and insulitis. Furthermore, in the absence of a key negative regulatory molecule, Cbl-b, 100% of mice develop autoimmunity upon infection with viruses encoding the lower-affinity ligand. Therefore, autoimmune disease is sensitive both to the affinity of the activating ligand and to normal mechanisms that negatively regulate the immune response. [ABSTRACT FROM AUTHOR]

Published

2004

10. Complement component C3 promotes T-cell priming and lung migration to control acute influenza virus infection.

Author

Kopf, Manfred, Abel, Brian, Gallimore, Awen, Carroll, Michael, and Bachmann, Martin F.

Subjects

COMPLEMENT (Immunology), T cells, INFLUENZA

Abstract

The complement cascade defines an important link between the innate and the specific immune system. Here we show that mice deficient for the third component of complement (C3-/- mice) are highly susceptible to primary infection with influenza virus. C3-/- mice showed delayed viral clearance and increased viral titers in lung, whereas mice deficient for complement receptors CR1 and CR2 (Cr2-/- mice) cleared the infection normally. Priming of T-helper cells and cytotoxic T cells (CTLs) in lung-draining lymph nodes was reduced, and the recruitment into the lung of virus-specific CD4+ and CD8+ effector T cells producing interferon-γ was severely impaired in C3-/- but not in Cr2-/- mice. Consequently, T-helper cell?dependent IgG responses were reduced in C3-/- mice but remained intact in Cr2-/- mice. These results demonstrate that complement induces specific immunity by promoting T-cell responses. [ABSTRACT FROM AUTHOR]

Published

2002

11. Deletion of the CD4 silencer element supports a stochastic mechanism of thymocyte lineage commitment.

Author

Leung, Ray K. M., Thomson, Kirsty, Gallimore, Awen, Jones, Emma, Van den Broek, Maries, Sierro, Sophie, Alsheikhly, Abdul-Razzak, McMichael, Andrew, and Rahemtulla, Amin

Subjects

MEDICAL genetics, GENE expression

Abstract

The mechanism of T cell lineage commitment remains controversial; to examine it we deleted the CD4-silencer element in the germ line of a mouse using a combination of gene targeting and Cre/LoxP-mediated recombination. We found that these mice were unable to extinguish CD4 expression either in immature thymocytes or mature CD8+ cytotoxic T cells (CTLs), which resulted in the development of major histocompatibility complex class II?restricted double-positive CTLs in the periphery. This finding strongly supports a stochastic over an instructive mechanism of coreceptor down-regulation. [ABSTRACT FROM AUTHOR]

Published

2001

12. HIV-specific cytotoxic T-cells in HIV-exposed but uninfected Gambian women.

Author

Rowland-Jones, Sarah, Sutton, Julian, Ariyoshi, Koya, Dong, Tao, Gotch, Frances, McAdam, Steve, Whitby, Denise, Sabally, Sehu, Gallimore, Awen, Corrah, Tumani, Takiguchi, Masafumi, Schultz, Thomas, McMichael, Andre, and Whittle, Hilton

Published

1995

13. The MHC E locus in macaques is polymorphic and is conserved between macaques and humans.

Author

Boyson, Jonathan, McAdam, Stephen, Gallimore, Awen, Golos, Thaddeus, Liu, Xiaomin, Gotch, Frances, Hughes, Austin, and Watkins, David

Abstract

Although the functions of the molecules encoded by the classical MHC class I loci are well defined, no function has been ascribed to the molecules encoded by the non-classical MHC class I loci. To investigate the evolution and conservation of the non-classical loci, we cloned and sequenced HLA-E homologues in macaques. We isolated four E locus alleles from five rhesus monkeys and two E locus alleles from one cynomolgus monkey, which indicated that the E locus in macaques is polymorphic. We also compared the rate of nucleotide substitution in the second intron of the macaque and human E locus alleles with that of exons two and three. The rate of nucleotide substitution was significantly higher in the introns, which suggested that the E locus has evolved under selective pressure. Additionally, comparison of the rates of synonymous and non-synonymous substitutions in the peptide binding region versus the remainder of the molecule suggested that the codons encoding the amino acids in the peptide binding region had been conserved in macaques and humans over the 36 million years since macaques and humans last shared a common ancestor. [ABSTRACT FROM AUTHOR]

Published

1995

14. Early suppression of SIV replication by CD8+ nef-specific cytotoxic T cells in vaccinated macaques.

Author

Gallimore, Awen, Cranage, Martin, Cook, Nicola, Almond, Neil, Bootman, Janet, Ruo, Erling, Silvera, Pete, Dennis, Michael, Corcoran, Terry, Stott, Jim, Mcmichael, Andrew, and Gotch, Frances

Published

1995